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Patrick An Introduction to Medicinal Chemistry 3/e Chapter 19 CHOLINERGICS, ANTICHOLINERGICS

Patrick An Introduction to Medicinal Chemistry 3/e Chapter 19 CHOLINERGICS, ANTICHOLINERGICS & ANTICHOLINESTERASES Part 2: Cholinergics & anticholinesterases. Contents Part 2: Cholinergics & anticholinesterases 12. Cholinergic Antagonists (Muscarinic receptor) (2 slides)

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Patrick An Introduction to Medicinal Chemistry 3/e Chapter 19 CHOLINERGICS, ANTICHOLINERGICS

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  1. Patrick An Introduction to Medicinal Chemistry 3/e Chapter 19 CHOLINERGICS, ANTICHOLINERGICS & ANTICHOLINESTERASES Part 2: Cholinergics & anticholinesterases

  2. Contents Part 2: Cholinergics & anticholinesterases 12. Cholinergic Antagonists (Muscarinic receptor) (2 slides) 12.1. Atropine 12.2. Hyoscine (scopolamine) 12.3. Comparison of atropine with acetylcholine 12.4. Analogues of atropine 12.5. Simplified Analogues (2 slides) 12.6. SAR for Antagonists (3 slides) 12.7. Binding Site for Antagonists (2 slides) 13. Cholinergic Antagonists (Nicotinic receptor) 13.1. Curare (2 slides) 13.2. Binding 13.3. Analogues of tubocurarine (5 slides) [22 slides]

  3. Ach Ach Antagonist Ach Postsynaptic nerve Postsynaptic nerve 12. Cholinergic Antagonists (Muscarinic receptor) • Drugs which bind to cholinergic receptor but do not activate it • Prevent acetylcholine from binding • Opposite clinical effect to agonists - lower activity of • acetylcholine

  4. 12. Cholinergic Antagonists (Muscarinic receptor) • Clinical Effects • Decrease of saliva and gastric secretions • Relaxation of smooth muscle • Decrease in motility of GIT and urinary tract • Dilation of pupils • Uses • Shutting down digestion for surgery • Ophthalmic examinations • Relief of peptic ulcers • Treatment of Parkinson’s Disease • Anticholinesterase poisoning • Motion sickness

  5. easily racemised 12. Cholinergic Antagonists (Muscarinic receptor) 12.1 Atropine • Racemic form of hyoscyamine • Source - roots of belladonna (1831) (deadly nightshade) • Used as a poison • Used as a medicine decreases GIT motility antidote for anticholinesterase poisoning dilation of eye pupils • CNS side effects - hallucinations

  6. 12. Cholinergic Antagonists (Muscarinic receptor) 12.2 Hyoscine (scopolamine) • Source - thorn apple • Medical use - treatment of motion sickness • Used as a truth drug (CNS effects)

  7. 12. Cholinergic Antagonists (Muscarinic receptor) 12.3 Comparison of atropine with acetylcholine • Relative positions of ester and nitrogen similar in both molecules • Nitrogen in atropine is ionised • Amine and ester are important binding groups (ionic + H-bonds) • Aromatic ring of atropine is an extra binding group (vdW) • Atropine binds with a different induced fit - no activation • Atropine binds more strongly than acetylcholine

  8. Ipratropium (bronchodilator & anti-asthmatic) Atropine methonitrate (lowers GIT motility) 12. Cholinergic Antagonists (Muscarinic receptor) 12.4 Analogues of atropine • Analogues are fully ionised • Analogues unable to cross the blood brain barrier • No CNS side effects

  9. Amprotropine Tridihexethyl bromide Propantheline chloride 12. Cholinergic Antagonists (Muscarinic receptor) 12.5 Simplified Analogues Pharmacophore = ester + basic amine + aromatic ring

  10. 12. Cholinergic Antagonists (Muscarinic receptor) 12.5 Simplified Analogues Benztropine (Parkinsons disease) Tropicamide (opthalmics) Cyclopentolate (opthalmics) Pirenzepine (anti-ulcer) Benzhexol (Parkinsons disease)

  11. R' = Aromatic or Heteroaromatic 12. Cholinergic Antagonists (Muscarinic receptor) 12.6 SAR for Antagonists • Important features • Tertiary amine (ionised) or a quaternary nitrogen • Aromatic ring • Ester • N-Alkyl groups (R) can be larger than methyl (unlike agonists) • Large branched acyl group • R’ = aromatic or heteroaromatic ring • Branching of aromatic/heteroaromatic rings is important

  12. Active Inactive 12. Cholinergic Antagonists (Muscarinic receptor) 12.6 SAR for Antagonists

  13. SAR for Antagonists SAR for Agonists 12. Cholinergic Antagonists (Muscarinic receptor) 12.6 SAR for Antagonists vs. Agonists Quaternary nitrogen Aromatic ring Ester N-Alkyl groups = methyl R’ = H Tertiary amine (ionised) or quaternary nitrogen Aromatic ring Ester N-Alkyl groups (R) can be larger than methyl R’ = aromatic or heteroaromatic Branching of Ar rings important

  14. van der Waals binding regions for antagonists Acetylcholine binding site RECEPTOR SURFACE 12. Cholinergic Antagonists (Muscarinic receptor) 12.7 Binding Site for Antagonists

  15. 12. Cholinergic Antagonists (Muscarinic receptor) 12.7 Binding Site for Antagonists

  16. Tubocurarine 13. Cholinergic Antagonists (Nicotinic receptor) • 13.1 Curare • Extract from ourari plant • Used for poison arrows • Causes paralysis (blocks acetylcholine signals to muscles) • Active principle = tubocurarine

  17. 13. Cholinergic Antagonists (Nicotinic receptor) • Pharmacophore • Two quaternary centres at specific separation (1.15nm) • Different mechanism of action from atropine based antagonists • Different binding interactions • Clinical uses • Neuromuscular blocker for surgical operations • Permits lower and safer levels of general anaesthetic • Tubocurarine used as neuromuscular blocker but side effects

  18. protein complex (5 subunits) diameter=8nm S 8nm 9-10nm a) Receptor dimer b) Interaction with tubocurarine Tubocurarine Acetylcholine binding site 13. Cholinergic Antagonists (Nicotinic receptor) 13.2 Binding

  19. Decamethonium Suxamethonium 13. Cholinergic Antagonists (Nicotinic receptor) 13.3 Analogues of tubocurarine • Long lasting • Long recovery times • Side effects on heart • Esters incorporated • Shorter lifetime (5 min) • Fast onset and short duration • Side effects at autonomic ganglia

  20. Pancuronium (R=Me) Vecuronium (R=H) 13. Cholinergic Antagonists (Nicotinic receptor) 13.3 Analogues of tubocurarine • Steroid acts as a spacer for the quaternary centres (1.09nm) • Acyl groups are added to introduce the Ach skeleton • Faster onset then tubocurarine but slower than suxamethonium • Longer duration of action than suxamethonium (45 min) • No effect on blood pressure and fewer side effects

  21. 13. Cholinergic Antagonists (Nicotinic receptor) 13.3 Analogues of tubocurarine Atracurium • Design based on tubocurarine and suxamethonium • Lacks cardiac side effects • Rapidly broken down in blood both chemically and metabolically • Avoids patient variation in metabolic enzymes • Lifetime is 30 minutes • Administered as an i.v. drip • Self destruct system limits lifetime

  22. INACTIVE 13. Cholinergic Antagonists (Nicotinic receptor) 13.3 Analogues of tubocurarine ACTIVE Atracurium stable at acid pH Hofmann elimination at blood pH (7.4)

  23. 13. Cholinergic Antagonists (Nicotinic receptor) 13.3 Analogues of tubocurarine Mivacurium • Faster onset (2 min) • Shorter duration (15 min)

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